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利用 PTSD 和心血管疾病的大规模遗传学研究来证明稳健的共同风险,并提高风险预测准确性。

Leveraging Large-Scale Genetics of PTSD and Cardiovascular Disease to Demonstrate Robust Shared Risk and Improve Risk Prediction Accuracy.

机构信息

Department of Psychiatry, Harvard Medical School, Boston (Seligowski, Misganaw, Ressler, Guffanti); McLean Hospital, Belmont, Mass. (all authors).

出版信息

Am J Psychiatry. 2022 Nov 1;179(11):814-823. doi: 10.1176/appi.ajp.21111113. Epub 2022 Sep 7.

Abstract

OBJECTIVE

Individuals with posttraumatic stress disorder (PTSD) are significantly more likely to be diagnosed with cardiovascular disease (CVD) (e.g., myocardial infarction, stroke). The evidence for this link is so compelling that the National Institutes of Health convened a working group to determine gaps in the literature, including the need for large-scale genomic studies to identify shared genetic risk. The aim of the present study was to address some of these gaps by utilizing PTSD and CVD genome-wide association study (GWAS) summary statistics in a large biobank sample to determine the shared genetic risk of PTSD and CVD.

METHODS

A large health care biobank data set was used (N=36,412), combined with GWAS summary statistics from publicly available large-scale PTSD and CVD studies. Disease phenotypes (e.g., PTSD) were collected from electronic health records. De-identified genetic data from the biobank were genotyped using Illumina SNP array. Summary statistics data sets were processed with the following quality-control criteria: 1) SNP heritability h >0.05, 2) compute z-statistics (z=beta/SE or z=log(OR)/SE), 3) filter nonvariable SNPs (0<freq<1), and 4) filter SNPs with low number of samples. The multitrait analysis of GWAS (MTAG) approach was used to combine GWAS summary statistics.

RESULTS

Significant genetic correlations were found between PTSD and CVD (r=0.24, SE=0.06), and Mendelian randomization analyses indicated a potential causal link from PTSD to hypertension (β=0.20, SE=0.04), but not the reverse. PTSD summary statistics significantly predicted PTSD diagnostic status (R=0.27), and this was significantly improved by incorporating summary statistics from CVD and major depressive disorder (R=1.30). Further, pathway enrichment analyses indicated that genetic variants involved in shared PTSD-CVD risk included those involved in postsynaptic structure, synapse organization, and interleukin-7-mediated signaling pathways.

CONCLUSIONS

The results from this study suggest that PTSD and CVD may share genetic risk. Further, these results implicate PTSD as a risk factor leading to the development of hypertension and coronary artery disease. Additional research is needed to determine the clinical utility of these findings.

摘要

目的

患有创伤后应激障碍(PTSD)的个体更有可能被诊断患有心血管疾病(CVD)(例如心肌梗死、中风)。这一联系的证据如此确凿,以至于美国国立卫生研究院召集了一个工作组来确定文献中的差距,包括需要进行大规模基因组研究以确定共同的遗传风险。本研究的目的是通过利用 PTSD 和 CVD 全基因组关联研究(GWAS)汇总统计数据在大型生物库样本中确定 PTSD 和 CVD 的共同遗传风险来解决其中的一些差距。

方法

使用了大型医疗保健生物库数据集(N=36412),并结合了来自公开的大型 PTSD 和 CVD 研究的 GWAS 汇总统计数据。疾病表型(例如 PTSD)是从电子健康记录中收集的。生物库中的匿名遗传数据使用 Illumina SNP 芯片进行基因分型。汇总统计数据数据集经过以下质量控制标准进行处理:1)SNP 遗传力 h >0.05,2)计算 z 统计量(z=beta/SE 或 z=log(OR)/SE),3)过滤非变异 SNP(0<freq<1),4)过滤样本数量低的 SNP。使用多性状 GWAS(MTAG)方法来组合 GWAS 汇总统计数据。

结果

发现 PTSD 和 CVD 之间存在显著的遗传相关性(r=0.24,SE=0.06),孟德尔随机化分析表明 PTSD 与高血压之间存在潜在的因果关系(β=0.20,SE=0.04),但反之则不然。PTSD 汇总统计数据显著预测 PTSD 诊断状态(R=0.27),通过纳入 CVD 和重度抑郁症的汇总统计数据,这一预测得到了显著改善(R=1.30)。此外,途径富集分析表明,与 PTSD-CVD 风险相关的遗传变异包括那些与突触后结构、突触组织和白细胞介素-7 介导的信号通路相关的遗传变异。

结论

本研究的结果表明,PTSD 和 CVD 可能具有共同的遗传风险。此外,这些结果表明 PTSD 是导致高血压和冠心病发展的危险因素。需要进一步研究来确定这些发现的临床实用性。

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